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United States Patent |
5,705,168
|
Parab
|
January 6, 1998
|
Enhanced permeation of alpha-hydroxy acid enantiomer
Abstract
Methods of increasing the rate of lactic acid permeation in skin for the
treatment of dermatological disorders by applying a composition containing
an inorganic or organic salt of lactic acid in a dermatologically
acceptable composition wherein at least 70% of the lactic acid moiety in
the salt is L-lactic acid, and compositions for practicing such methods.
Inventors:
|
Parab; Prakash (Williamsville, NY)
|
Assignee:
|
Bristol-Myers, Squibb Company (New York, NY)
|
Appl. No.:
|
452444 |
Filed:
|
May 26, 1995 |
Current U.S. Class: |
424/401; 514/557; 514/844; 514/846 |
Intern'l Class: |
A61K 007/00; A61K 031/19 |
Field of Search: |
424/401
514/557,553,844,846
|
References Cited
U.S. Patent Documents
4021572 | May., 1977 | Van Scott | 424/317.
|
4360523 | Nov., 1982 | Kaplan | 424/257.
|
4363815 | Dec., 1982 | Yu | 424/274.
|
4863506 | Sep., 1989 | Young | 71/113.
|
5091171 | Feb., 1992 | Yu | 424/642.
|
5254343 | Oct., 1993 | Parab | 424/401.
|
Primary Examiner: Kishore; Gollamudi S.
Attorney, Agent or Firm: Simon; Morton S.
Parent Case Text
This application is a divisional of application Ser. No. 08/215,985, filed
Mar. 22, 1994 now abandoned.
Claims
What is claimed is:
1. A dermatological composition comprising an inorganic or organic lactate
in a dermatologically acceptable carrier, from about 70% to about 100% of
the lactate being an L-lactate salt.
2. The composition as claimed in claim 1 wherein the lactate is an organic
lactate.
3. The composition as claimed in claim 2 wherein the lactate is a lactate
of an amino acid.
4. The composition as claimed in claim 3 wherein the amino acid is selected
from the group consisting of lysine and histidine.
5. The composition as claimed in claim 1, 2, 3 or 4 wherein the composition
has a pH of 2.5 to 9.
6. The composition as claimed in claim 1, 2, 3 or 4 wherein at least about
85% of the lactate is the L-lactic anion.
7. The composition as claimed in claim 1, 2, 3 or 4 wherein the composition
has a pH of from about 3.5 to 7 and at least about 85% of the lactate is
the L-lactic anion.
8. The composition as claimed in claim 1 wherein lactate is an inorganic
lactate.
9. The composition as claimed in claim 8 wherein the lactate is selected
from the group consisting of ammonium, sodium and potassium lactates.
10. The composition as claimed in claim 8 or 9 wherein the composition has
a pH of from 2.5 to 9.
11. The composition as claimed in claim 8 or 9 wherein at least about 85%
of the lactate is the L-lactic anion.
12. The composition as claimed in claim 8 or 9 wherein the composition has
a pH of from about 3.5 to 7 and at least about 85% of the lactate is the
L-lactic anion.
Description
FIELD OF THE INVENTION
This invention relates to topical administration of therapeutic
compositions for the treatment of determatological disorders, to
compositions employed for such administration and to methods of preparing
such compositions. More particularly, it relates to topical administration
of therapeutically effective amounts of L-lactic acid salts under
conditions such that there is rapid and higher skin permeation of the
L-lactic acid.
BRIEF DESCRIPTION OF THE PRIOR ART
The topical use of .alpha.-hydroxy acids and .alpha.-keto acids for the
treatment of various skin conditions is well known in the art. It is
described, for example in U.S. Pat. Nos. 3,879,537, 4,105,783 and
4,363,815.
U.S. Pat. No. 5,091,171 describes the employment of salts of various
.alpha.-hydroxyacids and .alpha.-keto acids with amines, especially
amphoteric amines, including amino acids, dipeptides, polypeptides and
proteins. Typical therapeutically useful salts described in the patent
include, for example, lysine lactate, a salt obtained by reaction between
lysine and the .alpha.-hydroxyacid, lactic acid. Other salts include
aliphatic, aromatic and heterocyclic amino acids; dibasic and diacidic
amino acids; substituted and unsubstituted amino acids as well as
synthetic and natural amino acids. The prior art recognizes that
.alpha.-hydroxy acids exist in enantiomeric forms and racemic mixtures,
but there is no recognition of a distinction between the skin permeation
and, hence, the therapeutic efficacy of the enantiomers and racemic
mixtures. More specifically, there is no recognition in the prior art of
the discovery described and claimed herein, namely that the L-form of
lactic acid is more efficient for permeating mammalian skin than is the
D-form.
BRIEF DESCRIPTION OF THE DRAWINGS
FIGS. 1 and 2 are graphs which will assist in understanding the improved
properties of the compositions and methods of this invention.
SUMMARY OF THE INVENTION
Novel compositions and methods for the treatment of dermatological
disorders have now been discovered. The compositions comprise a
dermatologically effective amount of a salt of L-lactic acid together with
a dermatologically acceptable topical carrier. The most preferred
compositions are substantially free of salts of D-lactic acid. More
specifically, the salt of lactic acid in such compositions is
substantially only in the L-form. However, as will be explained more fully
hereinafter, compositions containing a salt of L-lactic acid and a salt of
D-lactic acid are useful provided at least about 70% of the lactic acid
component in such compositions is in the L-form.
Generally, the pH of the novel compositions is such as to permit salt
formation with the inorganic or organic base employed. Optimum pH,
therefore will depend upon the basicity of the selected salt forming base.
Usually, the pH of the composition will be from about 2.5 to 9, preferably
3.5 to 7 and most preferably from 4 to 5.5. These pH ranges permit salt
formation with preferred bases.
It has been further discovered that topical administration of a composition
of the present invention to patients in need of such administration
promotes more rapid permeation of the lactic acid into the skin and a
higher concentration of lactic acid in the skin during observed time
periods.
The compositions employed in this invention are useful for all known
utilities for topical administration of .alpha.-hydroxyacids. These
include, for example, treatment of dry skin, xerosis, ichthyosis,
dandruff, acne, keratoses, psoriasis, wrinkles, warts, blemished skin,
eczema, age spots, laxity, leathery texture, roughness, sallow complexion,
scaling, telangiectasia, mottled pigment, skin atrophy caused by steroids,
hyperpigmented skin, inflammatory dermatoses, skin changes associated with
intrinsic ageing and photodamage, and skin cleansing.
In addition to the L-lactic acid salt, the compositions of the invention
may contain any of a large number of auxiliary cosmetic and pharmaceutical
agents, provided that such additional agents are inert with respect to the
formation, stability and activity of the L-lactic acid salts of the
invention, i.e., they are reaction inert.
Cosmetic and pharmaceutical agents include those that improve or eradicate
age spots, keratoses and wrinkles; analgesics; anesthetics; antiacne
agents; antibacterials; antiyeast agents; antifungal agents; antiviral
agents; antidandruff agents; antidermatitis agents; antipruritic agents;
antiinflammatory agents; antihyperkeratolytic agents; antidryskin agents;
antiperspirants; antipsoriatic agents; antiseborrheic agents; hair
conditioners and hair treatment agents; antiaging and antiwrinkle agents;
antiphotoaging agents; antiasthmatic agents and bronchodilators; sunscreen
agents; antihistamine agents; skin lightening agents; depigmenting agents;
vitamins; corticosteroids; tanning agents; hormones; retinoids; topical
cardiovascular agents and other dermatologicals.
Examples of typical cosmetic and pharmaceutical agents are clotrimazole,
ketoconazole, miconazole, griseofulvin, hydroxyzine, diphenhydramine,
pramozine, lidocaine, procaine, mepivacaine, monobenzone, erythromycin,
tetracycline, clindamycin, meclocycline, hydroquinone, 4-hydroxyanisole,
minocycline, naproxen, ibuprofen, theophylline, cromolyn, albuteral, all
trans retinoic acid, 13-cis retinoic acid, hydrocortisone, hydrocortisone
21-acetate, hydrocortisone 17-valerate, hydrocotisone 17-butyrate,
betamethasone valerate, betamethasone dipropionate, triamcinolone
acetonide, fluocinonide, clobetasol propionate, halobetasol propionate,
benzoyl peroxide, crotamiton, propranolol, promethazine, vitamin A
palmitate, vitamin E acetate and calcipotriene.
The term "dermatological disorders", as used herein, refers to any of those
mentioned above as well as other conditions treated by cosmetologists or
dermatologists with .alpha.-hydroxy acids or salts thereof. It includes
skin conditions the treatment of which might usually be regarded as
cosmetic, such as treatment of hyperpigmented skin areas, as well as more
serious skin conditions such as chronic and acute psoriasis.
The salts of this invention may be employed with any of a variety of
dermatologically acceptable carriers or excipients normally employed with
compositions for topical administration. These are well known to the
skilled artisan and include, for example, surfactants, emulsifiers,
stabilizers, preservatives, antiseptics, emollients, thickeners,
lubricants, humectants, chelating agents, fragrances and skin permeation
enhancers.
The compositions may be in the form of solutions, emulsions, suspensions,
lotions, creams, gels, ointments, liposomes, aerosol sprays, polymeric
gels, sticks, plasters, patches, films or tapes, the preparation of which
are well known to those skilled in the art of topical formulations.
Examples of suitable emulsifiers include, steareth-2, steareth-21,
polyoxyethylene-4-lauryl ether, polyethylene glycol-23-lauryl ether,
sorbitan monostearate and polyoxyethylene-20-sorbitan monostearate.
Examples of preservatives include, methyl paraben, propyl paraben, sorbic
acid, potassium sorbate, benzyl alcohol, diazolidinyl urea,
methylisothiazolinone and methylchloroisothiazolinone.
Examples of emollients include, silicone oils, mineral oil, cocoa butter,
hexyl laurate, diisopropyl adipate, dibutyl adipate, glyceryl stearate,
beeswax, lanolin, sperm wax, cetyl palmitate, isopropyl myristate,
isopropyl palmitate, isopropyl isostearate and propylene glycol
dioctanoate.
Among the thickening agents there may be mentioned, by way of example,
xanthan gum brine tolerant (xanthan gum BT), xanthan gum and gum acacia,
all of which are excellent as emulsion stabilizers and gelling agents.
Acceptable humectants include, for example, propylene glycol, glycerin,
butylene glycol and polyethylene glycols.
As will be recognized by the skilled artisan, the term "effective amount"
relates to the condition under treatment. Some conditions may require
treatment with large amounts of L-lactic acid salts. Others may be
effectively treated with smaller amounts. The treatment may require one or
multiple dosage units applied all at once or over a period of time.
Generally, the dosage requirements will be of the order of magnitude
normally employed with similar treatments using .alpha.-hydroxyacids.
However, because of the rapid onset of permeation and higher permeation
concentration achieved, it is often possible to use lesser amounts of
.alpha.-hydroxy acid salts in accordance with the procedures of this
invention. In any event, the skilled artisan will have no difficulty in
determining an "effective amount" for the treatment of a specific
condition, by the application of the routine test procedures normally
employed.
DETAILED DESCRIPTION OF THE INVENTION
The advantages of this invention will be readily apparent from the
following description taken together with the results illustrated in the
figures.
The compositions tested are shown in the following Table 1. The
formulations in this table and subsequent tables are represented by
capital letters. Those represented by the same letter in different tables
are identical formulations.
The compositions were prepared by mixing the identified forms of the lactic
acid and the selected amino acid together with water until uniform. The
mixture was heated to a temperature of 60.degree.-65.degree. C. with
mixing for 25 minutes. Mixing was continued while cooling to room
temperature and the necessary amount of water was added. The pH was then
measured.
TABLE 1
______________________________________
Composition of solution formulations containing L-lysine and L-
histidine salts of 12% DL and L-lactic acid.
Ingredients A B C D
______________________________________
DL-Lactic Acid (88%)
13.6 13.6 -- --
L-Lactic Acid (88%)
-- -- 13.6 13.6
L-Histidine 16.52 -- 16.52 --
L-Lysine Monohydrate
-- 16.14 -- 16.14
Water QS 100.00 100.00 100.00
100.00
pH 4.75 4.63 4.81 4.69
______________________________________
The capacity of the various compositions to penetrate the epidermis was
tested by the following standard procedure.
In-vitro Skin Permeation Study
.sup.14 C-L-lactic acid sodium salt and .sup.14 C-DL-lactic acid sodium
salt were used in the skin permeation study. The formulations with
L-lactic acid salts and DL-lactic acid salts were spiked with .sup.14
C-L-lactic acid sodium salt and .sup.14 C-DL-lactic acid sodium salt,
respectively, to result in a radioactive concentration of 6 micro curie
per ml.
Skin Preparation
Excised human cadaver skin samples obtained from the New York Firefighters
Skin Bank were used. The skin was supplied as sterile, split-thickness
skin with most of the underlying dermis already removed. The skin samples
were thawed for 15 minutes at room temperature and then transferred and
rinsed in normal saline for 30 minutes. Appropriate size specimens were
sectioned into squares to fit the diffusion cells.
Franz Diffusion Cell Study at Finite Dose
For each formulation, the skin section was mounted on three or four flat
flange Franz diffusion cells (FDC 400) with a diffusional cross-section
area of 1.2 cm.sup.2. A 100 micro liter sample of test formulation was
placed on the stratum corneum surface of the skin in the donor compartment
and the receptor compartment was filled with about 11 ml of normal saline.
The receptor fluid was well stirred throughout the experiment and the
temperature was maintained by circulating water at 37.degree. C. through
the water jacket of the diffusion cells. Precisely 500 .mu.l of receptor
fluid was collected in a scintillation vial at appropriate intervals over
a period of about 73 hours. Fifteen ml of scintillation fluid (INSTA-GEL
XF, PACKARD) were added directly to the scintillation vial and the lactic
acid content was determined on a Beckman LS 3801 scintillation counter.
The receptor fluid was replenished after each withdrawal. All the receptor
fluid and replenished fluids were filtered using a 0.22 .mu.m filter and
thoroughly degassed before use.
FIG. 1 shows the results of a skin permeation study comparing compositions
containing:
12% solution of the L-histidine salt of DL-lactic acid
12% solution of the L-lysine salt of DL-lactic acid
12% solution of the L-lysine salt of L-lactic acid
It will be seen that over the course of about 70 hours, the permeation of
DL-lactic acid (DL-LA), whether as a salt with L-histidine (L-His) or with
L-lysine (L-Lys), was essentially the same. In contrast, over the complete
course of the study, the degree of permeation of L-lactic acid (L-LA) as a
salt with L-lysine was rapid in onset and much higher than with the other
compositions.
Table 2 summarizes the results shown in FIG. 1. From the table, it is clear
that at 4 hours and 73 hours, the skin permeation of L-lactic acid (as the
L-lysine salt) is about 7.5 fold and 2 fold higher than that of the
corresponding DL-lactic acid salt. It is also clear that L-lactic acid
permeated faster and to a higher level than DL-lactic acid from their
respective L-lysine salt solutions and that there is practically no
difference in the permeation profile of the DL-lactic acid from either the
L-lysine or L-histidine lactate solutions.
TABLE 2
______________________________________
In vitro skin permeation of L-lactic acid and DL-lactic acid from
different formulations.
Amount Permeated Amount permeated relative
(mcg/cm.sup.2) to DL-LA-L-Lysine control
Formulation
4 Hours 73 Hours 4 Hours 73 Hours
______________________________________
B 21 119 1.0 1.0
D 158 223 7.5 1.9
A 18 143 0.9 1.2
______________________________________
Similar results are achieved if the L-lactic acid salts are prepared from
either enantiomer of histidine or lysine or from racemic mixtures of these
amino acids. The essence of the invention is the L-lactic acid anion not
the geometric arrangement of the atoms in the cation.
FIG. 2 shows the results of a further study comparing:
12% solution of the L-Histidine salt of DL-lactic acid
12% solution of the L-Histidine salt of L-lactic acid
12% solution of the L-Lysine salt of L-lactic acid.
It is again seen that there is a rapid onset of permeation and a
consistently higher degree of permeation for the L-lactic acid as a salt
of L-histidine compared to DL-lactic acid as a salt of L-histidine.
Table 3 summarizes the results shown in FIG. 2. From the table, it is clear
that at 4 hours and 73 hours, the skin permeation of L-lactic acid (as the
L-histidine salt) is about 10.3 fold and 2.1 fold higher than that of the
corresponding DL-lactic acid salt. Overall the rank order of skin
permeation is L-LA-L-His>L-LA-L-Lys>DL-LA-L-His. In each instance, the
L-lactic acid salt has higher degree of permeation and more rapid onset
than DL-lactic acid salt.
The permeation of L-lactic acid can be further improved in comparison to
DL-lactic acid by selecting appropriate cations. The NH.sub.4.sup.+,
Na.sup.30 , K.sup.+, cations are preferred over L-lysine and L-histidine,
because of their small molecular weight compared to amino acids, because
they are more readily available and because they provide consistently good
results.
TABLE 3
______________________________________
In vitro skin permeation of L-lactic acid and DL-lactic acid from
different formulations
Amount Permeated Amount permeated relative
(mcg/cm.sup.2) to DL-LA-L-His control
Formulation
4 Hours 73 Hours 4 Hours 73 Hours
______________________________________
A 23 631 1.0 1.0
C 237 1309 10.3 2.1
D 293 994 12.7 1.6
______________________________________
It will be noted by a comparison of the second columns in Tables 2 and 3
that there are appreciable differences in the amounts of permeated
products under what appear to be identical conditions. This apparent
anomaly arises because different skin samples were employed in the tests.
The skilled artisan will know that there are large variations in skin
porosity and that tests of the nature employed herein are only valid when,
as here, identical skin samples are compared.
The salts of this invention may be obtained by standard procedures by
reaction between L-lactic acid and any of variety of inorganic alkali and
organic bases.
Any of a wide variety of inorganic alkali bases or organic bases may be
employed to form the inorganic and organic salts of this invention, and
such salts will be prepared by simple acid/base reactions using procedures
well known to the skilled artisan. Alkali and alkaline earth metal salts,
such as Na, K, Ca, Mg and Li hydroxides, oxides, carbonates, bicarbonates
and others may be utilized. Ammonium salts, particularly ammonium
hydroxide, are useful as are quaternary ammonium compounds such as
tri-alkylammonium hydroxide. Organic nitrogen bases, including both
natural and synthetic amino acids, peptides, polypeptides, and proteins,
are useful. Other nitrogen containing bases which may be employed to
produce the salts include, organic bases with imino, guanidino,
imidazolino, imidazolyl, or other equivalent functionality. Various
primary, secondary and tertiary amines, particularly those substituted
with C.sub.1-8 alkyl or aryl groups, may be utilized. Preferred amines
include, alkanolamines mono-, di- and tri-substituted amines such as
propyl and dipropyl amine, aniline, methyl aniline and propyl aniline,
pryridine, dialkanolamines, alkylalkanolamines, trialkylamines and
trialkanolamines.
The useful salts of the invention also include amphoteric salts of L-lactic
acid, such as, lecithin, phosphotidyl ethanolamine, phosphatidyl serine
and sphingomyelin salts. They also include salts prepared from ornithine,
arginine, carnosine (alanyl-histidine), 4-aminobutanoic acid and
citrulline (.alpha.-amino .alpha.-ureidovaleric acid).
Representative amino acid salts of lactic acid include, for example,
glycine, alanine, valine, leucine, isoleucine, serine, threonine,
cysteine, cystine and tryptophan. The most preferred are salts of the
basic amino acids lysine, histidine and arginine.
The important criterion in selecting the counter ion of the salts of the
invention is that the base from which they are formed have a low PK.sub.b
value. The base must be a sufficiently strong to counteract the acidity of
lactic acid. Lactic acid is a weak acid. A 1M aqueous solution of lactic
acid has a pH of 1.9. As stated above, the pH of the compositions of this
invention is such as to ensure salt formation. Generally, it is from about
2.5 to 9. Preferably it is from 3.5 to 7 and most preferably it is from 4
to 5.5.
The concentration of L-lactic acid salt in the enantiomer mixtures of the
invention is at least about 70%. Preferably it is 85%. Most preferably, it
is about 100%, i.e. the compositions are substantially free of D-lactic
acid salts.
The crux of this invention is the unexpected discovery that L-lactic acid,
as the sole lactic acid component, or in a mixture containing both
L-lactic acid and D-lactic acid, when in the form of selected salts of
either enantiomer, permeates mammalian skin at a higher rate than D-lactic
acid. Thus, when a topical mixture containing a major portion of an
L-lactic acid and a minor portion of a D-lactic acid is applied to human
skin, the L-lactic acid salt permeates the skin at a higher rate than the
D-lactic acid salt. As a result the proportion of L-lactic acid salt in
the skin compared to the D-lactic acid salt will be higher than the
proportion of these enantiomers in the form of their salts in the
composition.
The most preferred compositions of this invention will contain 100% of the
selected lactic acid salt in the L-form. However, there is a tendency for
pure L-lactic acid to spontaneously racemize with time to form an
equilibrium mixture containing about 85% of the L-enantiomer and about 15%
of the D-enantioner. Such mixtures are useful to form the compositions of
this invention.
At the present time, lactic acid is commercially available in solutions
containing 85 to 90% lactic acid in the D-form, or in the L-form or as a
racemic mixture. It is most convenient to use these solutions for the
preparation of compositions of this invention. The solutions can be mixed
in accordance with procedures readily apparent to the skilled artisan to
produce lactic acid solutions with a preselected proportion of L-lactic
acid and then converted to the selected salt. Thus, for example, an
L-lactic acid solution can be mixed with a DL-lactic acid solution to
prepare a solution containing 70% L-lactic acid and 30% D-lactic acid.
These mixtures are useful for the formation of the compositions of the
invention. They can be used directly or can be converted by well known
means to dermatological compositions of the invention such as lotions,
creams, ointments and the like, for topical administration to patients in
need of treatment for dermatological disorders.
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